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Most cited article - PubMed ID 11704646

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Article

The Dose-Dependent Effects of Multifunctional Enkephalin Analogs on the Protein Composition of Rat Spleen Lymphocytes, Cortex, and Hippocampus; Comparison with Changes Induced by Morphine

Ujcikova, Hana
Author Ujcikova, Hana ORCID Laboratory of Neurochemistry, Institute of Physiology of the Czech Academy of Sciences, Videnska 1083, 14220 Prague, Czech Republic
Roubalova, Lenka
Author Roubalova, Lenka Laboratory of Neurochemistry, Institute of Physiology of the Czech Academy of Sciences, Videnska 1083, 14220 Prague, Czech Republic
Lee, Yeon Sun
Author Lee, Yeon Sun ORCID Department of Pharmacology, University of Arizona, Tucson, AZ 85724, USA
Slaninova, Jirina
Author Slaninova, Jirina Laboratory of Neurochemistry, Institute of Physiology of the Czech Academy of Sciences, Videnska 1083, 14220 Prague, Czech Republic
Brejchova, Jana
Author Brejchova, Jana ORCID Laboratory of Neurochemistry, Institute of Physiology of the Czech Academy of Sciences, Videnska 1083, 14220 Prague, Czech Republic
Svoboda, Petr
Author Svoboda, Petr Laboratory of Neurochemistry, Institute of Physiology of the Czech Academy of Sciences, Videnska 1083, 14220 Prague, Czech Republic

Biomedicines. 2022 Aug 14 ; 10 (8) : . [epub] 20220814

ISSN 2227-9059
Source

This work aimed to test the effect of 7-day exposure of rats to multifunctional enkephalin analogs LYS739 and LYS744 at doses of 3 mg/kg and 10 mg/kg on the protein composition of rat spleen lymphocytes, brain cortex, and hippocampus. Alterations of proteome induced by LYS739 and LYS744 were compared with those elicited by morphine. The changes in rat proteome profiles were analyzed by label-free quantification (MaxLFQ). Proteomic analysis indicated that the treatment with 3 mg/kg of LYS744 caused significant alterations in protein expression levels in spleen lymphocytes (45), rat brain cortex (31), and hippocampus (42). The identified proteins were primarily involved in RNA processing and the regulation of cytoskeletal dynamics. In spleen lymphocytes, the administration of the higher 10 mg/kg dose of both enkephalin analogs caused major, extensive modifications in protein expression levels: LYS739 (119) and LYS744 (182). Among these changes, the number of proteins associated with immune responses and apoptotic processes was increased. LYS739 treatment resulted in the highest number of alterations in the rat brain cortex (152) and hippocampus (45). The altered proteins were functionally related to the regulation of transcription and cytoskeletal reorganization, which plays an essential role in neuronal plasticity. Administration with LYS744 did not increase the number of altered proteins in the brain cortex (26) and hippocampus (26). Our findings demonstrate that the effect of κ-OR full antagonism of LYS744 is opposite in the central nervous system and the peripheral region (spleen lymphocytes).

Keywords
chronic pain treatment, label-free quantification, morphine, multifunctional enkephalin analogs, proteomic analysis, rat brain, rat spleen lymphocytes,
Publication type
Journal Article MeSH

Article

Global changes in the rat heart proteome induced by prolonged morphine treatment and withdrawal

PloS one. 2012 ; 7 (10) : e47167. [epub] 20121009

PLoS One
ISSN 1932-6203
Source

Morphine belongs among the most commonly used opioids in medical practice due to its strong analgesic effects. However, sustained administration of morphine leads to the development of tolerance and dependence and may cause long-lasting alterations in nervous tissue. Although proteomic approaches enabled to reveal changes in multiple gene expression in the brain as a consequence of morphine treatment, there is lack of information about the effect of this drug on heart tissue. Here we studied the effect of 10-day morphine exposure and subsequent drug withdrawal (3 or 6 days) on the rat heart proteome. Using the iTRAQ technique, we identified 541 proteins in the cytosol, 595 proteins in the plasma membrane-enriched fraction and 538 proteins in the mitochondria-enriched fraction derived from the left ventricles. Altogether, the expression levels of 237 proteins were altered by morphine treatment or withdrawal. The majority of changes (58 proteins) occurred in the cytosol after a 3-day abstinence period. Significant alterations were found in the expression of heat shock proteins (HSP27, α-B crystallin, HSP70, HSP10 and HSP60), whose levels were markedly up-regulated after morphine treatment or withdrawal. Besides that morphine exposure up-regulated MAPK p38 (isoform CRA_b) which is a well-known up-stream mediator of phosphorylation and activation of HSP27 and α-B crystallin. Whereas there were no alterations in the levels of proteins involved in oxidative stress, several changes were determined in the levels of pro- and anti-apoptotic proteins. These data provide a complex view on quantitative changes in the cardiac proteome induced by morphine treatment or withdrawal and demonstrate great sensitivity of this organ to morphine.

MeSH
Substance Withdrawal Syndrome metabolism MeSH
Chaperonin 60 metabolism MeSH
Chaperonin 10 metabolism MeSH
Rats MeSH
Crystallins metabolism MeSH
Morphine pharmacology MeSH
Myocardium metabolism MeSH
Rats, Wistar MeSH
HSP27 Heat-Shock Proteins metabolism MeSH
HSP70 Heat-Shock Proteins metabolism MeSH
Proteome drug effects MeSH
Morphine Dependence MeSH
Animals MeSH
Check Tag
Rats MeSH
Male MeSH
Animals MeSH
Publication type
Journal Article MeSH
Research Support, Non-U.S. Gov't MeSH
Names of Substances
Chaperonin 60 MeSH
Chaperonin 10 MeSH
Crystallins MeSH
Morphine MeSH
HSP27 Heat-Shock Proteins MeSH
HSP70 Heat-Shock Proteins MeSH
Proteome MeSH

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